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Journal Article
Migration of human vascular smooth muscle cells involves serum-dependent repeated cytosolic calcium transients
A. Scherberich, M. Campos-Toimil, P. Ronde, K. Takeda, A. Beretz
Journal of Cell Science 2000 113: 653-662;
A. Scherberich
Pharmacologie et Physico-Chimie des Interactions Cellulaires et Moleculaires, UMR CNRS 7034, France.
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M. Campos-Toimil
Pharmacologie et Physico-Chimie des Interactions Cellulaires et Moleculaires, UMR CNRS 7034, France.
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P. Ronde
Pharmacologie et Physico-Chimie des Interactions Cellulaires et Moleculaires, UMR CNRS 7034, France.
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K. Takeda
Pharmacologie et Physico-Chimie des Interactions Cellulaires et Moleculaires, UMR CNRS 7034, France.
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A. Beretz
Pharmacologie et Physico-Chimie des Interactions Cellulaires et Moleculaires, UMR CNRS 7034, France.
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Summary

Migration of vascular smooth muscle cells (VSMC) is a key event in the formation of neointima during atherosclerosis. Fura-2 loaded VSMCs were used to investigate calcium homeostasis during cell migration. Multiple spontaneous transient increases in cytosolic free calcium [Ca(2+)](i)were observed in single human VSMCs migrating on type I collagen. Such [Ca(2+)](i)transients were dependent on the presence of serum or PDGF-BB. Removal of serum, or loading cells with BAPTA, abolished the transients and decreased cell migration speed. The transients were not affected by disruption of cell polarization by dihydrocytochalasin B. Adhesion was used to investigate the specific role of cell-substrate interactions in the generation of transients. Transients are seen in VSMCs adhering either on collagen or on poly-L-lysine, suggesting that generation of transients is not strictly dependent on integrins. Buffering [Ca(2+)](i) with BAPTA led to accumulation of (beta)1 integrins at the cellular tail, and to increased release of integrin on the extracellular matrix. These results demonstrate a role for [Ca(2+)](i) transients in the rapid, serum-dependent migration of VSMCs. These [Ca(2+)](i)transients are present in migrating VSMCs only when two simultaneous events occur: (1) substrate independent spreading and (2) stimulation of cells by serum components such as PDGF-BB.

  • © 2000 by Company of Biologists
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Journal Article
Migration of human vascular smooth muscle cells involves serum-dependent repeated cytosolic calcium transients
A. Scherberich, M. Campos-Toimil, P. Ronde, K. Takeda, A. Beretz
Journal of Cell Science 2000 113: 653-662;
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Journal Article
Migration of human vascular smooth muscle cells involves serum-dependent repeated cytosolic calcium transients
A. Scherberich, M. Campos-Toimil, P. Ronde, K. Takeda, A. Beretz
Journal of Cell Science 2000 113: 653-662;

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